八种肺癌异种移植模型中 2-氨基[3-11C]异丁酸和 2-氨基[11C]甲基异丁酸摄取的直接比较。
Direct comparison of 2‑amino[3‑11C]isobutyric acid and 2‑amino[11C]methyl‑isobutyric acid uptake in eight lung cancer xenograft models.
机构信息
Department of Molecular Imaging and Theranostics, National Institute of Radiological Sciences, National Institutes for Quantum and Radiological Science and Technology (QST‑NIRS), Chiba 263‑8555, Japan.
Department of Radiopharmaceuticals Development, National Institute of Radiological Sciences, National Institutes for Quantum and Radiological Science and Technology (QST‑NIRS), Chiba 263‑8555, Japan.
出版信息
Int J Oncol. 2018 Dec;53(6):2737-2744. doi: 10.3892/ijo.2018.4596. Epub 2018 Oct 16.
The non‑natural amino acid positron emission tomography tracers, 2‑amino[3‑11C]isobutyric acid ([3‑11C]AIB) and 2‑amino[11C]methyl‑isobutyric acid ([11C]MeAIB), are metabolically stable in vivo and accumulate in tumors. [3‑11C]AIB is transported into cells mainly via the amino acid transport system A and partially via systems L and ASC, whereas [11C]MeAIB is transported into cells specifically via system A. How transport via the different systems affects the tumor uptake of these tracers, however, is unclear. In the present study, the tumor uptake of the two tracers was directly compared in eight lung cancer models (A549, H82, H441, H460, H1299, H1650, PC14, and SY), and the correlation of tumor uptake with several factors (amino acid transporter expression, contribution of amino acid transport systems to AIB uptake and tumor proliferation indices) was analyzed. Biodistribution analyses revealed that the tumor uptake of [3‑11C]AIB (4.9 to 19.2% injected dose per gram [ID/g]) was higher than that of [11C]MeAIB (3.1 to 15.9% ID/g) in all eight tumors, with a statistically significant difference in three tumors (P<0.01 in H441 and H460 tumors, P<0.05 in H82 tumors). A significant correlation was observed between the tumor uptake of the two tracers (r=0.95, P<0.01). The mRNA expression levels of the amino acid transporters of system A (SLC38A1 and SLC38A2), system L (SLC7A5) and system ASC (SLC1A5) were higher in all eight tumors than in the normal lung, with widely varying expression patterns. Although the contributions of the amino acid transport systems, Ki‑67 indices and tumor doubling times greatly differed among the eight models, these factors did not correlate with the tumor uptake of either tracer. The higher tumor uptake of [3‑11C]AIB and the correlation of tumor uptake between [3‑11C]AIB and [11C]MeAIB warrant further investigation in clinical studies in order to clarify the role of [3‑11C]AIB PET in oncology imaging.
非天然氨基酸正电子发射断层扫描示踪剂 2-氨基[3-11C]异丁酸([3-11C]AIB)和 2-氨基[11C]甲基-异丁酸([11C]MeAIB)在体内代谢稳定,可在肿瘤中积聚。[3-11C]AIB 主要通过氨基酸转运系统 A 转运进入细胞,部分通过系统 L 和 ASC 转运,而[11C]MeAIB 则特异性通过系统 A 转运进入细胞。然而,不同系统的转运如何影响这些示踪剂在肿瘤中的摄取尚不清楚。在本研究中,直接比较了两种示踪剂在八种肺癌模型(A549、H82、H441、H460、H1299、H1650、PC14 和 SY)中的肿瘤摄取情况,并分析了肿瘤摄取与几个因素(氨基酸转运体表达、氨基酸转运系统对 AIB 摄取的贡献和肿瘤增殖指数)之间的相关性。生物分布分析显示,在所有八种肿瘤中,[3-11C]AIB(每克[ID/g]4.9 至 19.2%注射剂量)的肿瘤摄取量均高于[11C]MeAIB(3.1 至 15.9% ID/g),其中三种肿瘤的差异具有统计学意义(H441 和 H460 肿瘤中 P<0.01,H82 肿瘤中 P<0.05)。两种示踪剂的肿瘤摄取之间存在显著相关性(r=0.95,P<0.01)。所有八种肿瘤中的氨基酸转运体系统 A(SLC38A1 和 SLC38A2)、系统 L(SLC7A5)和系统 ASC(SLC1A5)的 mRNA 表达水平均高于正常肺,表达模式差异很大。尽管八种模型中的氨基酸转运系统、Ki-67 指数和肿瘤倍增时间的贡献差异很大,但这些因素与两种示踪剂的肿瘤摄取均无相关性。[3-11C]AIB 的肿瘤摄取较高,[3-11C]AIB 和[11C]MeAIB 之间的肿瘤摄取相关性,均值得进一步在临床研究中进行探讨,以阐明[3-11C]AIB PET 在肿瘤成像中的作用。
Zotero 插件